Serum erythropoietin in acute ischemic stroke: preliminary findings

Ischemic stroke is the most common stroke, caused by occlusion of cerebral vessels and leading causes of disability. Erythropoietin (EPO) has non-hematopoietic effects as a neuroprotectant after ischemic event. This study aimed to learn the serum level of EPO in acute ischemic stroke. This cross-sectional study of ischemic stroke patients with onset < 24 h and consecutive sampling was used to collect the data from medical records review, physical examinations, head CT, 24-h EPO, 24-h and seventh-day NIHSS. A total of 47 patients consisting of 59.6% women, with a median age of 53 years old (21–70). The median 24 h EPO level was 808.6 pg/mL (134.2–2988.9). The relationship between 24 h-EPO and 24-h NIHSS were not significant (r = 0.101; p = 0.250), nor to 7th day NIHSS (r =  − 0.0174; p = 0.121) and to delta NIHSS (r = 0.186; p = 0.106). The relationship of blood collection time (hour) and EPO was significant (r =  − 0.260; p = 0.039). There was a statistically significant difference between serum EPO levels in ischemic stroke patients with lacunar stroke compared to non-lacunar stroke (288.5 vs. 855.4 ng/mL; p = 0.021). There was a relationship between the time of collection of blood and the level of EPO and also there was difference EPO level in lacunar stroke subtype compared with non-lacunar. The relationship between EPO and NIHSS lost significance after analysis. There is a need for a future study comparing each stroke risk factor and the same blood collection time.


Ethical approval
Dr. Hasan Sadikin General Hospital Bandung Human Research Ethics Committee (LB.02.01/X/6.5.251.2019) had approved this study.This study had complied with all relevant ethical regulations (including The Declaration of Helsinki).

Result
A total of 124 subject with ischemic stroke was enrolled from August to December 2019, subjects were excluded due to other diseases, 11 subjects with > 24 h onset, five deaths, and nine subjects with hospital-acquired pneumonia.In the end, we recruited 47 patients (see supplementary material).Of the total subjects, 59.6% were women and, the median age was 53 (21-70) years.The level of hemoglobin, leukocyte, platelet, erythrocyte was normal compared to the reference value.Risk factor included hypertension (74.5%), hyperlipidemia (74.5%), diabetes mellitus (25.5%), hyperuricemia (10.6%) (Table 1).
This study showed median EPO 24 h 808.6 pg/mL, with a median 24 h NIHSS of 6 and 76.6% accounted for moderate stroke.The median of the seventh day NIHSS was seventh and, 85.1% accounted for a mild stroke.The median of delta NIHSS was 4, with 4.3% subject without changing NIHSS (Table 1).
This study also showed us that there was no significant relationship between comorbidities and other basic characteristics in lacunar and non-lacunar groups (p > 0.05) except increasing of total cholesterol and hypertrigliseride (Table 2).
Data analysis showed us that in 24-h, median EPO in mild stroke was 705.5 (159.9-2441.8)pg/mL and in moderate stroke was 822.5 (134.2-2988.9)pg/mL, but statistically, there was no significant difference.There was a statistically significant difference between serum EPO levels in ischemic stroke patients with lacunar stroke compared to nonlacunar stroke ( 288.5 vs. 855.4ng/mL; p = 0.021) (Table 4).
Data analysis showed us in seventh day, median EPO in mild stroke was 814.6 (134.2-2988.9)pg/mL and in moderate stroke was 428.3 (239.5-980)pg/mL, and statistically, there was no significant differentiation (Table 3 and Fig. 2).
The median blood collection time in this study was 12 (6-18) hours; data analysis showed a significant correlation between time to collect and EPO level, with a weak correlation and negative trend ( r = -0.260;p = 0.039) (Table 3 and Fig. 3).

Discussion
A total of 47 subjects was included in this study, acute ischemic stroke patients with 59.6% of women with the median age of 53 years.This data was similar with a characteristic patient of Sahlgrenska Academy Study on Ischemic Stroke (SAHLSIS) with a mean of 56 years.Hypertension and hyperlipidemia were the most common risk factor in this study, with hypertension could be a single risk factor and the most common risk factor for stroke 11,12 .
There was a positive trend of the relationship between 24 h EPO and delta NIHSS, but also statistically was not significant (r = 0.186, p = 0.106).This finding is consistent with a previous study from SAHLSIS that showed a negative relationship between 24 h EPO and Scandinavian Stroke Scale (SSS), but not significant statistically as well 11 .
Data analysis showed there was a negative correlation between blood collect time (hour) and EPO ( r = − 0.260; p = 0.039).There was no requirement time for exact blood collection time for this study, so the result for EPO might also be influenced.SAHLSIS study showed there is no significant differentiation between time (day) and EPO serum results 12 .
EPO serum could decrease in these situations such as chronic anemia, liver dysfunction, elderly, dementia but increase in hypoglycemia, head trauma or surgery history, hematologic disease, malignancy, atrial www.nature.com/scientificreports/fibrillation, congestive heart failure.All of the mentioned were exclusion criteria in this study, but retinal disease, hyperglycemia, hyperlipidemia were not excluded [13][14][15][16][17] .From this study results showed that there was no significant relationship between comorbidities and other basic characteristics in lacunar and non-lacunar groups (p > 0.05) except increasing of total cholesterol and hypertrigliseride.Some studies showed that EPO induces lipid catabolism activation via JAK2-STAT5 in adipose tissue, and later it produces triglycerides lipase (ATGL) so that decreased triglycerides serum level is expected, but there was no explanation on the relationship between cholesterol to EPO, according to this study there was a significant relationship between total cholesterol or triglyceride and EPO 18 .According to previously published results in chronic kidney disease patients, such inflammatory mediators as lipopolysaccharide and cytokines inhibit cholesterol efflux from cells by decreasing expression of the adenosine triphosphate-binding cassette A1 (ABCA1) gene.This effect leads to the decrease in reverse cholesterol transport and consequently the decrease in serum HDL-C levels.Furthermore, it was suggested that EPO expresses anti-inflammatory activities 19  research is needed for investigating correlation between EPO level and lipid metabolism in acute ischemic stroke patients.
Sex in this study was dominated by women (59.6%).In previous study showed that disability and quality of life in stroke women would be worse than men.That could be a bias factor for increasing NIHSS.Men will also have a 10% higher differentiation erythrocyte mass index than women related to hormonal factors, iron needs due to menstruation, pregnancy, and lactation 20 .
A total of 74.5% of subjects in this study had hypertension and, 25.5% with diabetes mellitus.This condition is related to chronic inflammation, which would induce immune activation such as T cell and monocyte which secreted pro-inflammatory cytokine interferon-gamma (IFN).This pro-inflammatory cytokine will influence the metabolism of iron in the bone marrow and decrease the sensitivity of EPO.On the other hand, this cytokine will increase the severity level of stroke and contribute to some bias for this study 18,[21][22][23][24] .
This study showed that the median level of 24-h EPO 808.6 pg/mL was higher than the SAHLSIS study (in Sweden population) with a mean of 9.3mIU/mL.There was a statistically significant difference between serum   www.nature.com/scientificreports/EPO levels in ischemic stroke patients with lacunar stroke compared to non-lacunar stroke (288.5 vs. 855.4ng/ mL; p = 0.021).Small lesions in lacunar stroke will certainly produce small ischemic lesions, this will result in a better clinical outcome in lacunar stroke than non-lacunar 25 .A wide brain damage also correlates with worsening of neurological deficit in acute ischemic stroke patients and wide ischemic changes were found in the non-lacunar group.This finding showed the extent of neuronal brain damage after ischemic stroke 5 .It should be borne in mind that lacunar infarcts are the stroke subtype with the best functional prognosis even in pure motor stroke, which is the lacunar syndrome with the greatest functional impairment, and we can asess using NIHSS on admission and discharge 24 .Tissue hypoxia and cerebral ischemia activate HIF-1α, which in turn activates transcription of the EPO and Vascular Endothelial Growth Factor (VEGF) genes.HIF-1α, EPO, and VEGF increased as early as 1 h after acute ischemic stroke and may be used as marker of severity of neuronal damage and recovery in brain ischemic.There were strong correlations between HIF-1α and on admission and discharge NIHSS 5 .The main targets of EPO are neurons, while VEGF prevents apoptosis and induces endothelial cell proliferation, resulting in angiogenesis and improved tissue oxygenation 5,26 .EPO also contributes to endothelial cell proliferation, and VEGF also has a direct neuroprotective effect on neuronal cells.EPO and VEGF receptors are also generated on microglial cells and astrocytes, the targets of which are glial cells, but the effect on neuronal survival is unclear.EPO is thought to be able to stop the signal for cell death thereby reducing infarct volume 14 .There is a need to study further the possible influence of environmental and gene interactions with EPO levels in acute ischemic stroke 24,27,28 .Due to stroke, HIF-1α and EPO starts to accumulate as a response to inadequate oxygen level.HIF-1α mRNA expression and EPO after hypoxia could be detected within first thirty to sixty minutes.The regulation of HIF-1α and EPO, in penumbra, is rising until 7.5 h after onset of ischemia, so blood collection time (less then 7.5 h onset) could influence the EPO level in acute ischemic stroke 5 .Therefore, a deeper understanding regarding the role of EPO, specifically in ischemic stroke, is required to improve recovery and brain repair process after stroke 29,30 .

Limitation of study
This study did not have the same blood collection time, and this study also did not compare each stroke risk factor in every subject.

Conclusion
There was a relationship between the time of collection of blood and the level of EPO and also there was difference EPO level in lacunar stroke subtype compared with non-lacunar.Future research using prospective method is needed regarding EPO level and clinical outcome in acute ischemic stroke comparing each stroke risk factor and the same blood collection time. https://doi.org/10.1038/s41598-024-53180-3

Table 1 .
. Further Characteristic of stroke patients.Data are number (%) or mean (standard deviation) or median (interquartile range).*normal distribution data presented with mean (SD), **non normal distribution data presented with median.

Table 2 .
Characteristic of stroke patients based on stroke subtype.Data are number (%) or mean (standard deviation) or median (interquartile range).*normal distribution data presented with mean (SD), **non normal distribution data presented with median.

Table 3 .
Correlation of EPO and NIHSS.Rank spearman was used for analysis.